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通过P物质/神经激肽K受体的嵌合形成来描绘速激肽受体亚型特异性所涉及的结构域。

Delineation of structural domains involved in the subtype specificity of tachykinin receptors through chimeric formation of substance P/substance K receptors.

作者信息

Yokota Y, Akazawa C, Ohkubo H, Nakanishi S

机构信息

Institute for Immunology, Kyoto University Faculty of Medicine, Japan.

出版信息

EMBO J. 1992 Oct;11(10):3585-91. doi: 10.1002/j.1460-2075.1992.tb05442.x.

Abstract

The mammalian tachykinin receptors belong to the family of G protein-coupled receptors and consist of the substance P, substance K and neuromedin K receptors (SPR, SKR and NKR). We constructed 14 chimeric receptors in which seven transmembrane segments were sequentially exchanged between the rat SPR and SKR and examined the subtype specificity of the chimeric receptors by radioligand binding and inositol phosphate measurements after transfection into COS cells. All chimeric receptors showed maximum responses in agonist-induced inositol phosphate stimulation. Detailed analysis of five receptors with agonist selectivity similar to SPR indicated that the selectivity is mainly determined by the region extending from transmembrane segment II to the second extracellular loop together with a minor contribution of the extracellular N-terminal portion. This conclusion was more directly confirmed by an additional chimeric formation in which the introduction of the above middle portion of SPR into the corresponding region of SKR conferred a high affinity binding to substance P. The tachykinin receptors can thus be divided into two functional domains: the region covering transmembrane segments V-VII and responsible for fundamental recognition of the common tachykinin sequence; and its preceding portion involved in evoking subtype specificity by interacting with the divergent sequences of the peptides.

摘要

哺乳动物速激肽受体属于G蛋白偶联受体家族,由P物质、K物质和神经介素K受体(SPR、SKR和NKR)组成。我们构建了14个嵌合受体,其中大鼠SPR和SKR的七个跨膜区段被依次交换,并在转染到COS细胞后通过放射性配体结合和肌醇磷酸测量来检测嵌合受体的亚型特异性。所有嵌合受体在激动剂诱导的肌醇磷酸刺激中均表现出最大反应。对五个具有类似于SPR的激动剂选择性的受体进行的详细分析表明,选择性主要由从跨膜区段II延伸到第二个细胞外环的区域决定,细胞外N端部分也有较小贡献。通过另外一种嵌合构建更直接地证实了这一结论,即将SPR的上述中间部分引入SKR的相应区域可赋予对P物质的高亲和力结合。因此,速激肽受体可分为两个功能域:覆盖跨膜区段V-VII并负责对常见速激肽序列进行基本识别的区域;以及通过与肽的不同序列相互作用而参与引发亚型特异性的其前面部分。

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